Hyperoxia/Hypoxia Exposure Primes a Sustained Pro-Inflammatory Profile of Preterm Infant Macrophages Upon LPS Stimulation

Nele Twisselmann; Julia Pagel; Axel Künstner; Markus Weckmann; Annika Hartz; Kirsten Glaser; Anne Hilgendorff; Wolfgang Göpel; Hauke Busch; Egbert Herting; Jason B Weinberg; Christoph Härtel

doi:10.3389/fimmu.2021.762789

Hyperoxia/Hypoxia Exposure Primes a Sustained Pro-Inflammatory Profile of Preterm Infant Macrophages Upon LPS Stimulation

Front Immunol. 2021 Nov 18:12:762789. doi: 10.3389/fimmu.2021.762789. eCollection 2021.

Authors

Nele Twisselmann¹, Julia Pagel^{1

2}, Axel Künstner³, Markus Weckmann^{4

5}, Annika Hartz¹, Kirsten Glaser⁶, Anne Hilgendorff⁷, Wolfgang Göpel¹, Hauke Busch³, Egbert Herting¹, Jason B Weinberg^{8

9}, Christoph Härtel¹⁰

Affiliations

¹ Department of Pediatrics, University of Lübeck and University Medical Center Schleswig-Holstein, Lübeck, Germany.
² Department of Infectious Diseases and Microbiology, University of Lübeck and University Medical Center Schleswig-Holstein, Lübeck, Germany.
³ Medical Systems Biology Group, Institute of Experimental Dermatology, University of Lübeck and University Medical Center Schleswig-Holstein, Lübeck, Germany.
⁴ Department of Pediatrics Pneumology & Allergology, University Medical Center Schleswig-Holstein, Lübeck, Germany.
⁵ Airway Research Center North (ARCN) , Member of the German Center for Lung Research (DZL), Lübeck, Germany.
⁶ Center for Pediatric Research, Division of Neonatology, Department of Women's and Children's Health, University of Leipzig Medical Centre, Leipzig, Germany.
⁷ Center for Comprehensive Developmental Care (CDeCLMU), Member of the German Center for Lung Research (DZL), Hospital of the Ludwig-Maximilians University (LMU), CPC-M bioArchive, Munich, Germany.
⁸ Department of Pediatrics, University of Michigan, Ann Arbor, MI, United States.
⁹ Department of Microbiology and Immunology, University of Michigan, Ann Arbor, MI, United States.
¹⁰ Department of Pediatrics, University of Würzburg, Würzburg, Germany.

Abstract

Preterm infants are highly susceptible to sustained lung inflammation, which may be triggered by exposure to multiple environmental cues such as supplemental oxygen (O₂) and infections. We hypothesized that dysregulated macrophage (MФ) activation is a key feature leading to inflammation-mediated development of bronchopulmonary dysplasia (BPD) in preterm infants. Therefore, we aimed to determine age-dependent differences in immune responses of monocyte-derived MФ comparing cord blood samples derived from preterm (n=14) and term (n=19) infants as well as peripheral blood samples from healthy adults (n=17) after lipopolysaccharide (LPS) exposure. Compared to term and adult MФ, LPS-stimulated preterm MФ showed an enhanced and sustained pro-inflammatory immune response determined by transcriptome analysis, cytokine release inducing a RORC upregulation due to T cell polarization of neonatal T cells, and TLR4 surface expression. In addition, a double-hit model was developed to study pulmonary relevant exposure factors by priming MФ with hyperoxia (O₂ = 65%) or hypoxia (O₂ = 3%) followed by lipopolysaccharide (LPS, 100ng/ml). When primed by 65% O₂, subsequent LPS stimulation in preterm MФ led to an exaggerated pro-inflammatory response (e.g. increased HLA-DR expression and cytokine release) compared to LPS stimulation alone. Both, exposure to 65% or 3% O₂ together with subsequent LPS stimulation, resulted in an exaggerated pro-inflammatory response of preterm MФ determined by transcriptome analysis. Downregulation of two major transcriptional factors, early growth response gene (Egr)-2 and growth factor independence 1 (Gfi1), were identified to play a role in the exaggerated pro-inflammatory response of preterm MФ to LPS insult after priming with 65% or 3% O₂. Preterm MФ responses to LPS and hyperoxia/hypoxia suggest their involvement in excessive inflammation due to age-dependent differences, potentially mediated by downregulation of Egr2 and Gfi1 in the developing lung.

Keywords: bronchopulmonary dysplasia; hyperoxia; hypoxia; infection; macrophages; preterm infants; sustained inflammation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Bronchopulmonary Dysplasia / etiology
Cytokines / biosynthesis
Female
Gene Expression Profiling
Gestational Age
Humans
Infant, Newborn
Infant, Premature / immunology*
Inflammation / etiology*
Lipopolysaccharides / pharmacology*
Macrophages / drug effects*
Macrophages / immunology
Male
Oxygen / pharmacology*
Toll-Like Receptor 4 / physiology

Substances

Cytokines
Lipopolysaccharides
TLR4 protein, human
Toll-Like Receptor 4
Oxygen